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A novel method for study of the aggregation of protein induced by metal ion aluminum(III) using resonance Rayleigh scattering technique

机译:共振瑞利散射技术研究金属离子铝(III)诱导蛋白质聚集的新方法

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We present a novel method for the study of the aggregation of protein induced by metal ion aluminum(III) using resonance Rayleigh scattering (RRS) technique. In neutral Tris-HCl medium, the effect of this aggregation of protein results in the enhancement of RRS intensity and the relationship between the enhancement of the RRS signal and the Al concentration is nonlinear. On this basis, we established a new method for the determination of the critical induced-aggregation concentrations (C-CIAC) of metal ion Al(III) inducing the protein aggregation. Our results show that many factors, such as, pH value, anions, salts, temperature and solvents have obvious effects. We also studied the extent of aggregation and structural changes using ultra-violet spectrometry, protein intrinsic fluorescence and circular dichroism to further understand the exact mechanisms of the aggregation characteristics of proteins induced by metal ion Al(III) at the molecular level, to help us to develop effective methods to investigate the toxicity of metal ion Al, and to provide theoretical and quantitative evidences for the development of appropriate treatments for neurodementia such as Parkinson's disease, Alzheimer's disease and dementia related to dialysis. (c) 2007 Elsevier B.V. All rights reserved.
机译:我们提出了一种使用共振瑞利散射(RRS)技术研究金属离子铝(III)诱导的蛋白质聚集的新方法。在中性Tris-HCl介质中,这种蛋白质聚集的作用导致RRS强度增强,并且RRS信号增强与Al浓度之间的关系是非线性的。在此基础上,我们建立了测定金属离子Al(III)诱导蛋白质聚集的临界诱导聚集浓度(C-CIAC)的新方法。我们的结果表明,许多因素(例如pH值,阴离子,盐,温度和溶剂)均具有明显的影响。我们还使用紫外光谱,蛋白质固有荧光和圆二色性研究了聚集程度和结构变化,以进一步了解分子水平上金属离子Al(III)诱导的蛋白质聚集特征的确切机制,以帮助我们为研究金属离子铝的毒性开发有效的方法,并为开发神经性痴呆(如帕金森氏病,阿尔茨海默氏病和透析相关性痴呆)的适当疗法提供理论和定量证据。 (c)2007 Elsevier B.V.保留所有权利。

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